Proteomic changes associated with racial background and sepsis survival outcomes

Intra-abdominal infection is a common cause of sepsis, and intra-abdominal sepsis leads to 156000 U.S. deaths annually. African American/Black adults have higher incidence and mortality rates from sepsis compared to Non-Hispanic White adults. A limited number of studies have traced survival outcomes...

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Veröffentlicht in:Molecular omics 2022-12, Vol.18 (1), p.923-937
Hauptverfasser: Kapp, Kathryn L, Arul, Albert B, Zhang, Kevin C, Du, Liping, Yende, Sachin, Kellum, John A, Angus, Derek C, Peck-Palmer, Octavia M, Robinson, Ren A. S
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Sprache:eng
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Zusammenfassung:Intra-abdominal infection is a common cause of sepsis, and intra-abdominal sepsis leads to 156000 U.S. deaths annually. African American/Black adults have higher incidence and mortality rates from sepsis compared to Non-Hispanic White adults. A limited number of studies have traced survival outcomes to molecular changes; however, these studies primarily only included Non-Hispanic White adults. Our goal is to better understand molecular changes that may contribute to differences in sepsis survival in African American/Black and Non-Hispanic White adults with primary intra-abdominal infection. We employed discovery-based plasma proteomics of patient samples from the Protocolized Care for Early Septic Shock (ProCESS) cohort ( N = 107). We identified 49 proteins involved in the acute phase response and complement system whose expression levels are associated with both survival outcome and racial background. Additionally, 82 proteins differentially-expressed in survivors were specific to African American/Black or Non-Hispanic White patients, suggesting molecular-level heterogeneity in sepsis patients in key inflammatory pathways. A smaller, robust set of 19 proteins were in common in African American/Black and Non-Hispanic White survivors and may represent potential universal molecular changes in sepsis. Overall, this study identifies molecular factors that may contribute to differences in survival outcomes in African American/Black patients that are not fully explained by socioeconomic or other non-biological factors. Plasma proteomics identified proteins in various immune pathways that may contribute to racial/ethnic disparities in sepsis survival outcomes.
ISSN:2515-4184
2515-4184
DOI:10.1039/d2mo00171c